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Histone deacetylase inhibitors in clinical development.

机译:组蛋白脱乙酰酶抑制剂的临床开发。

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In addition to a variety of other novel agents, interest in histone deacetylase inhibitors (HDACIs) as antineoplastic drugs has recently accelerated and increasing numbers of these compounds have entered clinical trials in humans. HDACIs represent a prototype of molecularly targeted agents that perturb signal transduction, cell cycle-regulatory and survival-related pathways. Newer generation HDACIs have been introduced into the clinical arena that are considerably more potent on a molar basis than their predecessors and are beginning to show early evidence of activity, particularly in hematopoietic malignancies. In addition, there is an increasing appreciation of the fact that HDACIs may act through mechanisms other than induction of histone acetylation and, as in the case of other molecularly-targeted agents, it is conceivable that the ultimate role of HDACIs in cancer therapy will be as modulators of apoptosis induced by other cytotoxic agents. One particularly promising strategy involves attempts tocombine HDACIs with other novel agents to promote tumour cell differentiation or apoptosis. The present review focuses on recent insights into the mechanisms by which HDACIs exert their anticancer effects, either alone or in combination with other compounds, as well as attempts to translate these findings into the clinic.
机译:除了多种其他新型药物外,近来对组蛋白脱乙酰基酶抑制剂(HDACIs)作为抗肿瘤药的兴趣也有所提高,并且越来越多的这类化合物已进入人体临床试验。 HDACIs是干扰信号转导,细胞周期调控和存活相关途径的分子靶向药物的原型。新一代的HDACIs已被引入临床领域,在摩尔方面比其前任产品更为有效,并开始显示出早期活性证据,特别是在造血系统恶性肿瘤中。此外,人们越来越认识到HDACI可能通过除诱导组蛋白乙酰化以外的其他机制起作用,并且像其他分子靶向药物一样,可以想象HDACI在癌症治疗中的最终作用将是作为其他细胞毒性剂诱导的凋亡调节剂。一种特别有前途的策略涉及尝试将HDACI与其他新型药物结合以促进肿瘤细胞分化或凋亡。本综述着重于对HDACI单独或与其他化合物组合发挥抗癌作用的机制的最新见解,以及将这些发现转化为临床的尝试。

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